1 Clinical Colorectal Cancer Abby Siegel MD, MS COLON CANCER COLON CANCER 1. Epidemiology 2. Risk factors 3. Manifestations 4. Treatment
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Clinical Colorectal Cancer
Abby Siegel MD, MS
COLON CANCERCOLON CANCER1. Epidemiology2. Risk factors3. Manifestations4. Treatment
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1. EPIDEMIOLOGY
- Colorectal cancer is the third most common cancer in the United States
- About 150,000 new cases/year- Most cases in people over 50
Colorectal Cancer Incidence, 2008
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Colorectal Cancer Deaths, 2008
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EPIDEMIOLOGY
- Incidence rates high in U.S.,Europe, Australia
Increasing in Japan- Increasing in Japan- Low in China, Africa
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EPIDEMIOLOGY
- Changes in incidence rates over time and with migration may indicate role g yof environmental factors
2. RISK FACTORS: Protective
- Folic acid- Exercise- NSAIDS- ? Calcium/Vitamin D- ? Fiber
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NSAIDS
1) Cox-1 and Cox-2 inhibition1) Cox-1 and Cox-2 inhibition-Aspirin, Ibuprofen-Bleeding risk
2) Selective Cox-2 inhibition-Rofecoxib (Vioxx), -Celecoxib (Celebrex)-Thrombosis risk
RISK FACTORS: Increased risk with…
-Advanced age
-Inflammatory bowel disease
-Consumption of high-fat dietp g
-Personal or family history of colon cancer
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FAMILIAL SYNDROMES
• HNPCC• HNPCC– Hereditary non-polyposis colon cancer
• APC– Adenomatous polyposis colip yp
• Both usually autosomal dominant
HNPCC (Lynch Syndrome)Hereditary Non-Polyposis Colon Cancer
• 2-5% of colon cancers• Caused by mutations in• Caused by mutations in
mismatch repair genes• Tend to present in the right
colon• Often associated with
endometrial cancer inendometrial cancer in women
• Start screening at age 21
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By age 50By age 50 By age 70By age 70
HNPCC Increases the Risk ofColorectal Cancer
Population RiskPopulation Risk 0.2%0.2% 2%2%HNPCC RiskHNPCC Risk >25%>25% 80%80%
Gastroenterology Gastroenterology 1996;110:10201996;110:1020--77Int J CancerInt J Cancer 1999;81:2141999;81:214--88
By age 50By age 50 By age 70By age 70
HNPCC Increases the Risk of Endometrial Cancer
Population RiskPopulation Risk 0.2%0.2% 1.5%1.5%HNPCC RiskHNPCC Risk 20%20% 60%60%
Gastroenterology Gastroenterology 1996;110:10201996;110:1020--77Int J CancerInt J Cancer 1999;81:2141999;81:214--88
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HNPCC: Cancer Risks
100100
% with % with cancercancer
8080
6060
4040
2020
ColorectalColorectal 78%78%
Endometrial Endometrial 43%43%
Stomach Stomach 19%19%BiliBili 18%18%
Aarnio M et al. Aarnio M et al. Int J CancerInt J Cancer 64:430, 199564:430, 1995
2020
002020 4040 6060 808000
Age (years)Age (years)
Biliary tract Biliary tract 18%18%Urinary tract Urinary tract 10%10%Ovarian Ovarian 9%9%
APC Adenomatous Polyposis Coli
• Less than 1% of colon cancers• Caused by mutation of APC gene (5q21)• Also associated with duodenal cancers,
desmoid tumors, “CHRPE” (congenital hypertrophy of the retinal pigment epithelium)
• Start screening at puberty
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3. MANIFESTATIONS
1. Growth of cancer at primary site
2. Metastatic spread
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MANIFESTATIONS
1 Growth of cancer at primary site1. Growth of cancer at primary sitea. Asymptomatic/screeningb. Right sided syndromec. Left sided syndrome
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MANIFESTATIONS1 Growth of cancer at primary site1. Growth of cancer at primary site
i. Asymptomatic- Detected by screening test
- Fecal occult blood- Sigmoidoscopy- Colonoscopy- “Virtual” colonoscopy - Molecular techniques
Virtual Colonoscopy
Pickhardt et al. NEJM, 349 (23): 2191, 2003
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Screening summary
• Average risk: colonoscopy every 10• Average risk: colonoscopy every 10 years over age 50
• Family history: colonoscopy 10 years before index case
l i l l• Dysplastic polyps: repeat colonoscopy after 3 years
Screening, continued…
• APC: annual flexible sigmoidoscopy• APC: annual flexible sigmoidoscopy starting at age 11, colectomy when polyps develop
• HNPCC: colonoscopy at age 21, then every 1-2 years
• Inflammatory bowel disease: start 8 years after pancolitis, 12 years after distal disease
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MANIFESTATIONS1. Growth of cancer at primary site. G owt o ca ce at p a y s te
ii. Right sided syndrome
a) Ascending colon has thin wall, large diameter, distensibleb) Liquid fecal stream) Ch i bl d l lt i ic) Chronic blood loss results in iron
deficiency anemia***d) Obstruction unlikely
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MANIFESTATIONS1. Growth of cancer at primary site1. Growth of cancer at primary site
iii. Left sided syndromea) Descending colon wall thicker, less
distensibleb) More solid fecal streamc) Tumors tend to infiltrated) Bright red blood more commone) Obstruction more common
“Apple core lesion”
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COMPARISON RIGHT AND LEFT SIDED COLON CANCERS
Right LeftAnemia +++ +Occult bleeding +++ +Gross bleeding + +++Abd. Mass ++ +Change in bowel
habits+ +++
Obstruction + +++
Stage Stage 11 Colorectal CancerColorectal Cancer•• 23% of colorectal CA23% of colorectal CA23% of colorectal CA23% of colorectal CA•• Cancer has grown Cancer has grown
through the mucosa through the mucosa and invades the and invades the muscularismuscularis
•• Treatment: surgery to Treatment: surgery to remove the tumor and remove the tumor and some surrounding some surrounding lymph nodeslymph nodes
•• Survival: 93%Survival: 93%
Adapted from www.plwc.org, 2007
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Stage Stage 22 Colorectal CancerColorectal Cancer•• 31% of colorectal CA31% of colorectal CA•• Cancer grows Cancer grows beyond the beyond the
muscularis muscularis of the colon or of the colon or rectum but has not spread rectum but has not spread to the lymph nodesto the lymph nodes
•• Treatment (colon): surgery Treatment (colon): surgery +/+/-- adjuvant chemotherapyadjuvant chemotherapy+/+/-- adjuvant chemotherapyadjuvant chemotherapy
•• Survival: 72 to 85%Survival: 72 to 85%•• Treatment (rectal): surgery, Treatment (rectal): surgery,
radiation and chemoradiation and chemo
Adapted from www.plwc.org, 2007
Stage Stage 33 Colorectal CancerColorectal Cancer•• 26% of colorectal CA26% of colorectal CA•• Cancer has spread to the Cancer has spread to the
regional lymph nodesregional lymph nodes•• Treatment (colon): surgery Treatment (colon): surgery
and adjuvant and adjuvant chemotherapychemotherapy
•• Survival: 44 to 83%Survival: 44 to 83%•• Treatment (rectal): surgery, Treatment (rectal): surgery,
radiation and radiation and chemotherapychemotherapy
Adapted from www.plwc.org, 2007
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Stage Stage 4 4 Colorectal CancerColorectal Cancer•• 20% of colorectal CA20% of colorectal CA•• Cancer has spread toCancer has spread to•• Cancer has spread to Cancer has spread to
other areas of the bodyother areas of the body•• Treatment: chemotherapy. Treatment: chemotherapy.
Consider surgery of Consider surgery of primary lesion, especially primary lesion, especially if symptomaticif symptomatic
•• Surgery to remove Surgery to remove metastases (liver/lung) in metastases (liver/lung) in carefully selected patientscarefully selected patients
•• Survival: 8%Survival: 8%Source: UpToDate.com, 2007
PROGNOSIS depends on…
1 Hi t l i l f t1. Histological features- poor differentiation-vascular invasion
2. Depth of invasion3. Nodal involvement4. Genetic alterations
-18q LOH (bad), MSI (good), K-ras mutation (limits response to anti-EGFR antibodies)
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MANIFESTATIONS
Metastatic SpreadMetastatic Spread1. Lymphatics
Mesenteric nodesVirchow’s node
2. Hematogenous spreadLiver via portal circulation
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LIVER METASTASES
MANIFESTATIONS1. Pain (stretching capsule)2. Hepatomegaly, nodularity3. Elevated liver function tests
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4. TREATMENTS1. Surgery
L li d di (St I II III)-Localized disease (Stage I, II, III)-Try to remove isolated metastases
2. Radiation therapy -Rectal cancer-helps prevent local recurrencerecurrence
3. Pharmaceuticals-Stage III and IV disease
TREATMENT: Pharmaceuticals
1. 5-Fluorouracil i idi ti t b lit- pyrimidine antimetabolite
2. Irinotecan- topoisomerase inhibitorprevents re-ligation after cleavage of DNA by topoisomerase I
3. Oxaliplatin- alkylating agent, causes formation of bulky DNA adducts
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Exciting new biologics…
4 Bevacizumab4. Bevacizumab -Antibody against VEGF-May block angiogenesis and also stabilize leaky vasculature
5. Cetuximab, Panitumomab-Antibodies against EGFR-Binds to EGF receptor on tumor cells, prevents dimerization and cell signaling
Bevacizumab toxicities
• Bleeding• Bleeding• Thrombosis• Hypertension• Wound healing complications
H lf lif b t 3 k it t l t 2 h lf• Half life about 3 weeks; wait at least 2 half-lives before major surgery
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EGFR inhibition and rash
Correlating Survival With Skin Rash
14P = .0008* P = .0007*
G3G2G1G0
Surv
ival
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12P = .04*
P = .0002*
9923/CRC 9814/Pancreas9816/SCCHN
* Log-rank P value, grade 0 vs. grades 1-3
Saltz L et al. Proc Am Soc Clin Oncol 2003; 22:204 (abstract 817)Slide courtesy of Josep Tabernero, MD
0
2
0141/CRC
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Original Article
Cetuximab and Chemotherapy as Initial Treatment for Metastatic Colorectal Cancer
Eric Van Cutsem, M.D., Ph.D., Claus-Henning Köhne, M.D., Erika Hitre, M.D., Ph.D., Jerzy Zaluski, M.D., Chung-Rong Chang Chien, M.D., Anatoly Makhson, M.D., Ph.D.,
Geert D'Haens, M.D., Ph.D., Tamás Pintér, M.D., Robert Lim, M.B., Ch.B., György Bodoky, M.D., Ph.D., Jae Kyung Roh, M.D., Ph.D., Gunnar Folprecht, M.D., Paul Ruff, M.D., Christopher Stroh, Ph.D., Sabine Tejpar, M.D., Ph.D., Michael Schlichting, Dipl.-
Stat., Johannes Nippgen, M.D., and Philippe Rougier, M.D., Ph.D.
N Engl J MedVolume 360(14):1408-1417
April 2, 2009
P P P PPP P P PP PSunitinibSunitinib
VEGFRPDGFR EGFR
BevacizumabVEGF
Cetuximab, Panitumomab
Molecularly Targeted Therapy in Oncology
P P P P
Raf
Mek
Ras
P13K
AKT
STAT
mTOR
HIF-1α HIF-1β
Transcription Factors
PP P P P PP P
Sorafenib
SunitinibSorafenib
Sorafenib
CCI-779RAD001
GefitinibErlotinib
Nucleus
Transcription Factors
Cell proliferationAngiogenesis Metastases
Survival/↓Apoptosis
Slide courtesy of Wells Messersmith, MD
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Hazard Ratios for Progression-free and Overall Survival and Odds Ratios with Tumor Response, According to the Mutation Status of KRAS in the Tumor
Van Cutsem E et al. N Engl J Med 2009;360:1408-1417
P P P PPP P P PP PSunitinibSunitinib
VEGFRPDGFR EGFR
BevacizumabVEGF
Cetuximab, Panitumomab
Molecularly Targeted Therapy in Oncology
P P P P
Raf
Mek
Ras
P13K
AKT
STAT
mTOR
HIF-1α HIF-1β
Transcription Factors
PP P P P PP P
Sorafenib
SunitinibSorafenib
Sorafenib
CCI-779RAD001
GefitinibErlotinib
Nucleus
Transcription Factors
Cell proliferationAngiogenesis Metastases
Survival/↓Apoptosis
Slide courtesy of Wells Messersmith, MD
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TREATMENTPharmaceuticals
1. “Adjuvant” (after surgery) Curative goal in patients after complete resection
2. Palliation in patients with gross metastatic disease
3. “Neoadjuvant” (before surgery) Shrink tumors, then try to resect in limited metastatic disease
TREATMENT:Metastatic disease
• Systemic chemotherapy now has improved• Systemic chemotherapy now has improved survival for those with metastatic disease to about 2 years
• We now sometimes treat neoadjuvantly (before surgery), shrinking metastases and then surgically removing themthen surgically removing them
• This is important, because some of these “limited metastases” patients are cured!
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Trends in the Median Survival of Patients with Advanced Colorectal Cancer
Meyerhardt, J. A. et al. N Engl J Med 2005;352:476-487
Estimated drug costs for eight weeks of treatment for metastatic colorectal cancer
10000
15000
20000
25000
30000
Cost in $
0
5000
5FU Combo Antibody
Schrag, D. N Engl J Med 2004;351:317-319
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Conclusions:• Know HNPCC and APC—these may help you ow N CC a d C t ese ay e p you
prevent cancers in others• Understand how colon cancer commonly presents
(right versus left-sided), and common sites of spread
• Think about colon (or other GI) cancer in an older person with iron-deficiency anemia—don’t just p y jgive them iron!
• Don’t give up on those with metastatic disease with new treatment options and occasionally cures
• My email:
• Many thanks to Tom Garrett for many slides!